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2,4,6-三硝基甲苯还原过程中NAD(P)H:黄素单核苷酸氧化还原酶的失活

NAD(P)H:flavin mononucleotide oxidoreductase inactivation during 2,4,6-trinitrotoluene reduction.

作者信息

Riefler R Guy, Smets Barth F

机构信息

Department of Civil Engineering, Ohio University, Athens, Ohio 45701, USA.

出版信息

Appl Environ Microbiol. 2002 Apr;68(4):1690-6. doi: 10.1128/AEM.68.4.1690-1696.2002.

Abstract

Bacteria readily transform 2,4,6-trinitrotoluene (TNT), a contaminant frequently found at military bases and munitions production facilities, by reduction of the nitro group substituents. In this work, the kinetics of nitroreduction were investigated by using a model nitroreductase, NAD(P)H:flavin mononucleotide (FMN) oxidoreductase. Under mediation by NAD(P)H:FMN oxidoreductase, TNT rapidly reacted with NADH to form 2-hydroxylamino-4,6-dinitrotoluene and 4-hydroxylamino-2,6-dinitrotoluene, whereas 2-amino-4,6-dinitrotoluene and 4-amino-2,6-dinitrotoluene were not produced. Progressive loss of activity was observed during TNT reduction, indicating inactivation of the enzyme during transformation. It is likely that a nitrosodinitrotoluene intermediate reacted with the NAD(P)H:FMN oxidoreductase, leading to enzyme inactivation. A half-maximum constant with respect to NADH, K(N), of 394 microM was measured, indicating possible NADH limitation under typical cellular conditions. A mathematical model that describes the inactivation process and NADH limitation provided a good fit to TNT reduction profiles. This work represents the first step in developing a comprehensive enzyme level understanding of nitroarene biotransformation.

摘要

细菌能够通过还原硝基取代基,轻松转化2,4,6-三硝基甲苯(TNT),这种污染物在军事基地和弹药生产设施中经常被发现。在这项研究中,利用一种模型硝基还原酶,即NAD(P)H:黄素单核苷酸(FMN)氧化还原酶,对硝基还原动力学进行了研究。在NAD(P)H:FMN氧化还原酶的介导下,TNT迅速与NADH反应,生成2-羟基氨基-4,6-二硝基甲苯和4-羟基氨基-2,6-二硝基甲苯,而未生成2-氨基-4,6-二硝基甲苯和4-氨基-2,6-二硝基甲苯。在TNT还原过程中观察到活性逐渐丧失,表明在转化过程中酶失活。很可能是一种亚硝基二硝基甲苯中间体与NAD(P)H:FMN氧化还原酶发生反应,导致酶失活。测得相对于NADH的半最大常数K(N)为394微摩尔,这表明在典型的细胞条件下可能存在NADH限制。一个描述失活过程和NADH限制的数学模型与TNT还原曲线拟合良好。这项工作是在酶水平上全面理解硝基芳烃生物转化的第一步。

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本文引用的文献

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Responses of intracellular cofactors to single and dual substrate limitations.细胞内辅因子对单一和双重底物限制的反应。
Biotechnol Bioeng. 1996 Mar 20;49(6):690-9. doi: 10.1002/(SICI)1097-0290(19960320)49:6<690::AID-BIT11>3.0.CO;2-A.

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